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Antibody targeting intracellular oncogenic Ras mutants exerts anti-tumour effects after systemic administration

Authors
Shin, SM | Choi, DK | Jung, K | Bae, J | Kim, JS | Park, SW | Song, KH  | Kim, YS
Citation
Nature communications, 8. : 15090-15090, 2017
Journal Title
Nature communications
ISSN
2041-1723
Abstract
Oncogenic Ras mutants, frequently detected in human cancers, are high-priority anticancer drug targets. However, direct inhibition of oncogenic Ras mutants with small molecules has been extremely challenging. Here we report the development of a human IgG1 format antibody, RT11, which internalizes into the cytosol of living cells and selectively binds to the activated GTP-bound form of various oncogenic Ras mutants to block the interactions with effector proteins, thereby suppressing downstream signalling and exerting anti-proliferative effects in a variety of tumour cells harbouring oncogenic Ras mutants. When systemically administered, an RT11 variant with an additional tumour-associated integrin binding moiety for tumour tissue targeting significantly inhibits the in vivo growth of oncogenic Ras-mutated tumour xenografts in mice, but not wild-type Ras-harbouring tumours. Our results demonstrate the feasibility of developing therapeutic antibodies for direct targeting of cytosolic proteins that are inaccessible using current antibody technology.
DOI
10.1038/ncomms15090
PMID
28489072
Appears in Collections:
Journal Papers > Hospital > Clinical Trial Center
Ajou Authors
송, 기훈
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